TY - JOUR
T1 - Kidneys derived from mice transgenic for human complement blockers are protected in an in vivo model of hyperacute rejection
AU - Lazzeri, Massimo
AU - Mora, Marirosa
AU - Mulder, Lubbertus C.F.
AU - Marsicano, Giovanni
AU - Marinucci, Giovanni
AU - Boschi, Manuela
AU - Bruzzone, Paolo
AU - Alfani, Dario
AU - Cortesini, Raffaello
AU - Rossini, Mara
N1 - Funding Information:
This work was supported by the Corsorzio Interuniversitario per i Trapianti d'Organo.
PY - 1998/4
Y1 - 1998/4
N2 - Purpose: The major obstacle to successful discordant kidney xenotransplantation is hyperacute rejection (HAR). Complement plays a key role in the induction of HRA, defined by endothelial cell activation, loss of vascular integrity, hemorrhage and thrombosis. The activation of complement is tightly controlled by a number of species-specific regulatory proteins which inhibit, at different points, the cascade of events leading to the formation of the membrane attack complex (MAC). We have tested the hypothesis that kidneys derived from transgenic mice expressing two human complement inhibitors, Decay Accelerating Factor (hDAF) and Membrane Cofactor Protein (MCP), could be protected from human complement-mediated damage. Materials and Methods: Control and transgenic mice were perfused with human plasma by cannulation of the right jugular vein, at a perfusion rate of 10 μL./min. for two hours. Complement C3 deposition was detected on kidney sections by immunohistochemistry using specific FITC antibody. Complement-induced tissue damage was evaluated by histopathological examination. Results: Heavy deposition of complement C3 was observed on kidneys derived from perfused control mice. This was associated with a characteristic HAR pathology of severe interstitial hemorrhage, inflammatory reaction, loss of glomerula and tubuli structure. Kidneys derived from mice transgenic for hDAF or hMCP were partially protected from both complement C3 deposition and tissue damage. The expression of both hDAF and hMCP in double transgenic mice significantly increases the protection from human complement-mediated damage. Conclusion: A novel model of in vivo perfusion with human plasma has been adopted to recreate the initial event of HAR. Our data show that this murine model could be very valuable to determine the effect of transgenic human molecules in protecting vascularized organs from human complement attack.
AB - Purpose: The major obstacle to successful discordant kidney xenotransplantation is hyperacute rejection (HAR). Complement plays a key role in the induction of HRA, defined by endothelial cell activation, loss of vascular integrity, hemorrhage and thrombosis. The activation of complement is tightly controlled by a number of species-specific regulatory proteins which inhibit, at different points, the cascade of events leading to the formation of the membrane attack complex (MAC). We have tested the hypothesis that kidneys derived from transgenic mice expressing two human complement inhibitors, Decay Accelerating Factor (hDAF) and Membrane Cofactor Protein (MCP), could be protected from human complement-mediated damage. Materials and Methods: Control and transgenic mice were perfused with human plasma by cannulation of the right jugular vein, at a perfusion rate of 10 μL./min. for two hours. Complement C3 deposition was detected on kidney sections by immunohistochemistry using specific FITC antibody. Complement-induced tissue damage was evaluated by histopathological examination. Results: Heavy deposition of complement C3 was observed on kidneys derived from perfused control mice. This was associated with a characteristic HAR pathology of severe interstitial hemorrhage, inflammatory reaction, loss of glomerula and tubuli structure. Kidneys derived from mice transgenic for hDAF or hMCP were partially protected from both complement C3 deposition and tissue damage. The expression of both hDAF and hMCP in double transgenic mice significantly increases the protection from human complement-mediated damage. Conclusion: A novel model of in vivo perfusion with human plasma has been adopted to recreate the initial event of HAR. Our data show that this murine model could be very valuable to determine the effect of transgenic human molecules in protecting vascularized organs from human complement attack.
KW - Human complement inhibitors
KW - Hyperacute rejection
KW - Transgenic mice
KW - Xenotransplantation
UR - http://www.scopus.com/inward/record.url?scp=0031922025&partnerID=8YFLogxK
U2 - 10.1016/S0022-5347(01)63617-6
DO - 10.1016/S0022-5347(01)63617-6
M3 - Article
C2 - 9507885
AN - SCOPUS:0031922025
SN - 0022-5347
VL - 159
SP - 1364
EP - 1369
JO - Journal of Urology
JF - Journal of Urology
IS - 4
ER -